Deletion of Rptor in Preosteoblasts Reveals a Role for the Mammalian Target of Rapamycin Complex 1 (mTORC1) Complex in Dietary‐Induced Changes to Bone Mass and Glucose Homeostasis in Female Mice

Deletion of Rptor in Preosteoblasts Reveals a Role for the Mammalian Target of Rapamycin Complex 1 (mTORC1) Complex in Dietary‐Induced Changes to Bone Mass and Glucose Homeostasis in Female Mice

ABSTRACT The mammalian target of rapamycin complex 1 (mTORC1) complex is the major nutrient sensor in mammalian cells that responds to amino acids, energy levels, growth factors, and hormones, such as insulin, to control anabolic and catabolic processes. We have recently shown that suppression of th...

Full description

Bibliographic Details
Main Authors: Pawanrat Tangseefa, Sally K. Martin, Agnieszka Arthur, Vasilios Panagopoulos, Amanda J. Page, Gary A. Wittert, Christopher G. Proud, Stephen Fitter, Andrew C.W. Zannettino
Format: Article
Language:English
Published: Wiley 2021-05-01
Series:JBMR Plus
Subjects:
BONE MARROW ADIPOSE TISSUE
DIET‐INDUCED INSULIN RESISTANCE
DIET‐INDUCED OBESITY
mTORC1
PREOSTEOBLAST
Online Access:https://doi.org/10.1002/jbm4.10486
id doaj-508e5481eadc4aedbd5040ad51e6553d
record_format Article
spelling doaj-508e5481eadc4aedbd5040ad51e6553d2021-05-06T15:43:59ZengWileyJBMR Plus2473-40392021-05-0155n/an/a10.1002/jbm4.10486Deletion of Rptor in Preosteoblasts Reveals a Role for the Mammalian Target of Rapamycin Complex 1 (mTORC1) Complex in Dietary‐Induced Changes to Bone Mass and Glucose Homeostasis in Female MicePawanrat Tangseefa0Sally K. Martin1Agnieszka Arthur2Vasilios Panagopoulos3Amanda J. Page4Gary A. Wittert5Christopher G. Proud6Stephen Fitter7Andrew C.W. Zannettino8Adelaide Medical School, Faculty of Health and Medical Science University of Adelaide Adelaide South Australia AustraliaAdelaide Medical School, Faculty of Health and Medical Science University of Adelaide Adelaide South Australia AustraliaAdelaide Medical School, Faculty of Health and Medical Science University of Adelaide Adelaide South Australia AustraliaAdelaide Medical School, Faculty of Health and Medical Science University of Adelaide Adelaide South Australia AustraliaAdelaide Medical School, Faculty of Health and Medical Science University of Adelaide Adelaide South Australia AustraliaAdelaide Medical School, Faculty of Health and Medical Science University of Adelaide Adelaide South Australia AustraliaNutrition, Diabetes & Gut Health Program, Lifelong Health Theme, South Australian Health and Medical Research Institute Adelaide South Australia AustraliaAdelaide Medical School, Faculty of Health and Medical Science University of Adelaide Adelaide South Australia AustraliaAdelaide Medical School, Faculty of Health and Medical Science University of Adelaide Adelaide South Australia AustraliaABSTRACT The mammalian target of rapamycin complex 1 (mTORC1) complex is the major nutrient sensor in mammalian cells that responds to amino acids, energy levels, growth factors, and hormones, such as insulin, to control anabolic and catabolic processes. We have recently shown that suppression of the mTORC1 complex in bone‐forming osteoblasts (OBs) improved glucose handling in male mice fed a normal or obesogenic diet. Mechanistically, this occurs, at least in part, by increasing OB insulin sensitivity leading to upregulation of glucose uptake and glycolysis. Given previously reported sex‐dependent differences observed upon antagonism of mTORC1 signaling, we investigated the metabolic and skeletal effects of genetic inactivation of preosteoblastic‐mTORC1 in female mice. Eight‐week‐old control diet (CD)‐fed Rptorob−/− mice had a low bone mass with a significant reduction in trabecular bone volume and trabecular number, reduced cortical bone thickness, and increased marrow adiposity. Despite no changes in body composition, CD‐fed Rptorob−/− mice exhibited significant lower fasting insulin and glucose levels and increased insulin sensitivity. Upon high‐fat diet (HFD) feeding, Rptorob−/− mice were resistant to a diet‐induced increase in whole‐body and total fat mass and protected from the development of diet‐induced insulin resistance. Notably, although 12 weeks of HFD increased marrow adiposity, with minimal changes in both trabecular and cortical bone in the female control mice, marrow adiposity was significantly reduced in HFD‐fed Rptorob−/− compared to both HFD‐fed control and CD‐fed Rptorob−/− mice. Collectively, our results demonstrate that mTORC1 function in preosteoblasts is crucial for skeletal development and skeletal regulation of glucose homeostasis in both male and female mice. Importantly, loss of mTORC1 function in OBs results in metabolic and physiological adaptations that mirror a caloric restriction phenotype (under CD) and protects against HFD‐induced obesity, associated insulin resistance, and marrow adiposity expansion. These results highlight the critical contribution of the skeleton in the regulation of whole‐body energy homeostasis. © 2021 The Authors. JBMR Plus published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research.https://doi.org/10.1002/jbm4.10486BONE MARROW ADIPOSE TISSUEDIET‐INDUCED INSULIN RESISTANCEDIET‐INDUCED OBESITYmTORC1PREOSTEOBLAST
collection DOAJ
language English
format Article
sources DOAJ
author Pawanrat Tangseefa
Sally K. Martin
Agnieszka Arthur
Vasilios Panagopoulos
Amanda J. Page
Gary A. Wittert
Christopher G. Proud
Stephen Fitter
Andrew C.W. Zannettino
spellingShingle Pawanrat Tangseefa
Sally K. Martin
Agnieszka Arthur
Vasilios Panagopoulos
Amanda J. Page
Gary A. Wittert
Christopher G. Proud
Stephen Fitter
Andrew C.W. Zannettino
Deletion of Rptor in Preosteoblasts Reveals a Role for the Mammalian Target of Rapamycin Complex 1 (mTORC1) Complex in Dietary‐Induced Changes to Bone Mass and Glucose Homeostasis in Female Mice
JBMR Plus
BONE MARROW ADIPOSE TISSUE
DIET‐INDUCED INSULIN RESISTANCE
DIET‐INDUCED OBESITY
mTORC1
PREOSTEOBLAST
author_facet Pawanrat Tangseefa
Sally K. Martin
Agnieszka Arthur
Vasilios Panagopoulos
Amanda J. Page
Gary A. Wittert
Christopher G. Proud
Stephen Fitter
Andrew C.W. Zannettino
author_sort Pawanrat Tangseefa
title Deletion of Rptor in Preosteoblasts Reveals a Role for the Mammalian Target of Rapamycin Complex 1 (mTORC1) Complex in Dietary‐Induced Changes to Bone Mass and Glucose Homeostasis in Female Mice
title_short Deletion of Rptor in Preosteoblasts Reveals a Role for the Mammalian Target of Rapamycin Complex 1 (mTORC1) Complex in Dietary‐Induced Changes to Bone Mass and Glucose Homeostasis in Female Mice
title_full Deletion of Rptor in Preosteoblasts Reveals a Role for the Mammalian Target of Rapamycin Complex 1 (mTORC1) Complex in Dietary‐Induced Changes to Bone Mass and Glucose Homeostasis in Female Mice
title_fullStr Deletion of Rptor in Preosteoblasts Reveals a Role for the Mammalian Target of Rapamycin Complex 1 (mTORC1) Complex in Dietary‐Induced Changes to Bone Mass and Glucose Homeostasis in Female Mice
title_full_unstemmed Deletion of Rptor in Preosteoblasts Reveals a Role for the Mammalian Target of Rapamycin Complex 1 (mTORC1) Complex in Dietary‐Induced Changes to Bone Mass and Glucose Homeostasis in Female Mice
title_sort deletion of rptor in preosteoblasts reveals a role for the mammalian target of rapamycin complex 1 (mtorc1) complex in dietary‐induced changes to bone mass and glucose homeostasis in female mice
publisher Wiley
series JBMR Plus
issn 2473-4039
publishDate 2021-05-01
description ABSTRACT The mammalian target of rapamycin complex 1 (mTORC1) complex is the major nutrient sensor in mammalian cells that responds to amino acids, energy levels, growth factors, and hormones, such as insulin, to control anabolic and catabolic processes. We have recently shown that suppression of the mTORC1 complex in bone‐forming osteoblasts (OBs) improved glucose handling in male mice fed a normal or obesogenic diet. Mechanistically, this occurs, at least in part, by increasing OB insulin sensitivity leading to upregulation of glucose uptake and glycolysis. Given previously reported sex‐dependent differences observed upon antagonism of mTORC1 signaling, we investigated the metabolic and skeletal effects of genetic inactivation of preosteoblastic‐mTORC1 in female mice. Eight‐week‐old control diet (CD)‐fed Rptorob−/− mice had a low bone mass with a significant reduction in trabecular bone volume and trabecular number, reduced cortical bone thickness, and increased marrow adiposity. Despite no changes in body composition, CD‐fed Rptorob−/− mice exhibited significant lower fasting insulin and glucose levels and increased insulin sensitivity. Upon high‐fat diet (HFD) feeding, Rptorob−/− mice were resistant to a diet‐induced increase in whole‐body and total fat mass and protected from the development of diet‐induced insulin resistance. Notably, although 12 weeks of HFD increased marrow adiposity, with minimal changes in both trabecular and cortical bone in the female control mice, marrow adiposity was significantly reduced in HFD‐fed Rptorob−/− compared to both HFD‐fed control and CD‐fed Rptorob−/− mice. Collectively, our results demonstrate that mTORC1 function in preosteoblasts is crucial for skeletal development and skeletal regulation of glucose homeostasis in both male and female mice. Importantly, loss of mTORC1 function in OBs results in metabolic and physiological adaptations that mirror a caloric restriction phenotype (under CD) and protects against HFD‐induced obesity, associated insulin resistance, and marrow adiposity expansion. These results highlight the critical contribution of the skeleton in the regulation of whole‐body energy homeostasis. © 2021 The Authors. JBMR Plus published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research.
topic BONE MARROW ADIPOSE TISSUE
DIET‐INDUCED INSULIN RESISTANCE
DIET‐INDUCED OBESITY
mTORC1
PREOSTEOBLAST
url https://doi.org/10.1002/jbm4.10486
work_keys_str_mv AT pawanrattangseefa deletionofrptorinpreosteoblastsrevealsaroleforthemammaliantargetofrapamycincomplex1mtorc1complexindietaryinducedchangestobonemassandglucosehomeostasisinfemalemice
AT sallykmartin deletionofrptorinpreosteoblastsrevealsaroleforthemammaliantargetofrapamycincomplex1mtorc1complexindietaryinducedchangestobonemassandglucosehomeostasisinfemalemice
AT agnieszkaarthur deletionofrptorinpreosteoblastsrevealsaroleforthemammaliantargetofrapamycincomplex1mtorc1complexindietaryinducedchangestobonemassandglucosehomeostasisinfemalemice
AT vasiliospanagopoulos deletionofrptorinpreosteoblastsrevealsaroleforthemammaliantargetofrapamycincomplex1mtorc1complexindietaryinducedchangestobonemassandglucosehomeostasisinfemalemice
AT amandajpage deletionofrptorinpreosteoblastsrevealsaroleforthemammaliantargetofrapamycincomplex1mtorc1complexindietaryinducedchangestobonemassandglucosehomeostasisinfemalemice
AT garyawittert deletionofrptorinpreosteoblastsrevealsaroleforthemammaliantargetofrapamycincomplex1mtorc1complexindietaryinducedchangestobonemassandglucosehomeostasisinfemalemice
AT christophergproud deletionofrptorinpreosteoblastsrevealsaroleforthemammaliantargetofrapamycincomplex1mtorc1complexindietaryinducedchangestobonemassandglucosehomeostasisinfemalemice
AT stephenfitter deletionofrptorinpreosteoblastsrevealsaroleforthemammaliantargetofrapamycincomplex1mtorc1complexindietaryinducedchangestobonemassandglucosehomeostasisinfemalemice
AT andrewcwzannettino deletionofrptorinpreosteoblastsrevealsaroleforthemammaliantargetofrapamycincomplex1mtorc1complexindietaryinducedchangestobonemassandglucosehomeostasisinfemalemice
_version_ 1721456606287233024

Similar Items